TW475930B - Novel compound, its use and pharmaceutical composition comprising it - Google Patents
Novel compound, its use and pharmaceutical composition comprising it Download PDFInfo
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- TW475930B TW475930B TW085104270A TW85104270A TW475930B TW 475930 B TW475930 B TW 475930B TW 085104270 A TW085104270 A TW 085104270A TW 85104270 A TW85104270 A TW 85104270A TW 475930 B TW475930 B TW 475930B
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Landscapes
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- Hospice & Palliative Care (AREA)
- Otolaryngology (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
- Plural Heterocyclic Compounds (AREA)
- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
- Heterocyclic Carbon Compounds Containing A Hetero Ring Having Oxygen Or Sulfur (AREA)
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Description
475930 A7 B7 五、發明説明() 本發明有關式(I)化合物
式(I)中之環A未被取代或被取代及環B未被取代或被取代。 這些化合物具有有價値之藥理性質,且爲特別有效之神經 激肽1頡頹劑及物質P頡頗劑。 本發明特別有關那些式(I)化合物及其鹽,其中之環A 未被取代或被低級烷基、低級烷氧基、鹵素、硝基或三氟 甲基單取代及環B未被取代或被1-4個由低級烷基、羥基、 低級烷氧基、低級烷硫基、鹵素、硝基、氰基及三氟甲基 組成之一組中選出之取代基取代,有關這些化合物之製備 方法、含這些化合物之醫藥組成物、這些化合物在醫療人 類或動物體上之用途或在製備醫藥組成物上之用途。 經濟部中央標準局員工消費合作社印製 (請先閱讀背面之注意事項再填寫本頁) 由於本發明化合物含至少兩個光學活性碳原子,因此 可以立體異構物、立體異構物混合物以及(實質上)純非 鏡像異構物形式存在。本發明亦包括相當之立體異構物。 式(I)化合物偏愛爲式(la)之非鏡像異構形式: 本紙張尺度適用中國國家標準(CNS ) A4規格(210X 297公釐) -4- 475930 A7 B7 五、發明説明()
若沒有其它定義,上文及下文中使用之一般名詞具有 以下之意義。 氏級"一詞意指各含1至7個(含),較適宜者爲I 至4個(含)碳原子之相當之基及化合物。 低級烷基典型上爲甲基、乙基、正丙基、異丙基、正 丁基、異丁基、第二丁基、第三丁基或一相當之戊基、己 基或庚基自由基。較適宜者爲CrC4院基。 低級烷氧基典型上爲甲氧基、乙氧基、正丙氧基、異 丙氧基、正丁氧基、異丁氧基、第二丁氧基、第三丁氧基 或一相當之戊氧基、己氧基或庚氧基自由基。較適宜者爲 Ci-C4院氧基。 幽素典型上爲氟基、氯基或溴基,但亦可爲碘基。較 適宜者爲氯基。 經濟部中央標準局員工消費合作社印製 (請先閱讀背面之注意事項再填寫本頁) 式(I)化合物可爲鹽形式,較偏愛者爲醫藥上可接受之 鹽形式。酸加成鹽可用六氫吡啶環之鹼性中心生成。適合 之酸成份可爲,例如,強無機酸,典型上爲礦物酸(例如 硫酸、磷酸(如正磷酸))、氫鹵酸(例如鹽酸)、強有 機羧酸,典型上爲可被,例如,_素取代之低級烷羧酸 (像醋酸或三氟乙酸)、二羧酸,其可爲不飽和者(例如 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) 經濟部中央標準局員工消費合作社印製 475930 A7 B7 五、發明説明() 草酸、丙二酸、琥珀酸、順丁烯二酸、反丁烯二酸、酞酸 或對酞酸)、羥羧酸(例如抗壞血酸、羥乙酸、乳酸、蘋 果酸、酒石酸或檸檬酸)、胺基酸(例如天冬胺酸或麩胺 酸)或苯甲酸、或有機磺酸,典型上爲可被,例如,鹵素 取代之低級烷磺酸,典型上爲甲磺酸、或可被,例如,低 級院基取代之芳磺酸,典型上爲對甲苯磺酸。亦包括不適 合醫療用之鹽,但其可用於,例如,分離或純化式(I)之自 由化合物或其醫藥上可接受之鹽。只有醫藥上可接受之無 毒性鹽可用於醫療上,因此爲較偏愛之鹽。 式(I)化合物(包括其醫藥上可接受之鹽,在下文中總 是包括鹽)具有有價値之藥理性質。其特別作爲神經激肽1 (NK1)頡頗劑,因此可預防,尤其是,因物質P釋出引起之 病徵。 呼吸道內有感覺神經,其中含若干神經肽,特別是速 激肽及CGRP (與降鈣素基因有關之肽)。感覺神經之活化 造成神經肽在肺內局部釋出。主要的是釋出物質P及神經激 肽A,其引發一稱爲神經原發炎之急性發炎反應。此發炎反 應主要經由NK1受體活化進行且特別包括血管擴張、微血 管洩漏、發炎白血球之反射增進及黏液大量分泌。這些物 質P效應爲氣喘之典型病徵。 式(I)化合物之藥理作用係特別基於NK1受體之頡頑作 用。式(I)化合物亦可抑制神經原發炎以及速激肽誘發之支 氣管收縮。 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) I---------^^衣 訂 (請先閱讀背面之注意事項再填寫本頁) -6- 475930 A7 B7 五、發明説明() 式(I)化合物之有利效果可利用不同的體外或活體內試 驗方法證實。例如在有ED50値之天竺鼠活體內NK1支氣管 痙攣試驗,口服劑量由大約〇.〇3毫克/公斤有效,在靜脈注 射3.0 微克 /公斤[Sar9, Met(02)l 1]-物質P [= SarSP]前2、4 或24 小 時,施予測試物質。施用SarSP誘發天竺鼠之氣管內壓增 加。本發明化合物有顯著的口服活性以及長有效期。 經濟部中央標準局員工消費合作社印製 (請先閲讀背面之注意事項再填寫本頁) 式(I)化合物作爲NK1受體頡頡劑,在預防、治療或診 斷許多疾病上很有用,例如:上及下呼吸道疾病(像支氣 管性氣喘、過敏性氣喘、非過敏性氣喘、過敏性過敏及分 泌過多病症(如慢性支氣管炎及囊性纖維變性))、各種 病因之肺纖維變性、肺及支氣管循環疾病(像肺高血壓、 血管形成、轉移)、胃腸道疾病(像克隆氏病(Crohn’s disease)、希什斯普隆氏病(Hirsprung’s disease)、腹瀉、吸收不良 症、發炎症、中樞及周圍神經系統之精神性、外傷性或發 炎性分裂(像抑鬱、焦慮、偏頭痛及其它類型之頭痛、中 風、嘔吐)、血管疾病(例如頭顱血管疾病)、與各種組 織(像皮膚及眼睛)中微循環有關之疾病、免疫系統及網 狀內皮細胞組織系統疾病(例如在脾及淋巴組織中)、疼 痛病及其它疾病(涉及在其病因、病理及病原中神經激 肽、速激肽及其它有關物質之活性者)。 物質P爲一天然產生之速激肽族之十一肽。其產生於哺 乳動物器官中且在藥理上作爲神經肽。物質P在各種疾病中 扮演重要角色,例如在疼痛病、偏頭痛及一些中樞神經系 統之病症(像焦慮狀態、嘔吐、精神分裂症及抑鬱)以及 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) -7- 經濟部中央標準局員工消費合作社印製 475930 A7 B7 五、發明説明() 在一些運動的病症中,像在巴金生氏病(Parkinson’s disease) 中,也在發炎疾病中,像在風濕性關節炎、虹膜炎及結合 膜炎中,在呼吸器官疾病中,像在氣喘及慢性支氣管炎 中,在胃腸道疾病中,像在潰瘍性結腸炎及克隆氏病(Crohn’s disease)中,及在尚血壓中。 許多努力朝向提升物質P頡頡劑領域之發展及尋找,例 如,具有較廣範圍活性以及提高之活性及提高之生物利用 性以及增進之化學安定性及結晶性之適合之物質P頡頡劑。 廣泛的藥理試驗證實新穎化合物及其鹽能頡頑物質p至 一特別適宜的程度,因此特別適合治療物質P引起之病徵。 物質P-額頑效果可,如下文所述,用專家已知之試驗方 法檢測。此效果在體外以及活體內發現。在依照H.Bittiger, Ciba Foundation Symposium 91 (1982) 196 - 199 之放射性受體分析 中,式(I)化合物,例如,抑制3H物質P與牛視網膜之結合至 一出奇高的程度,具有大約5ι^Μ[起之IC5。値。
藥理數據(I): 3H物質P與牛視網膜結合之抑鬼L 實施例化 IC5〇 合物編號 [nM] 1/1 5.5 3/7 10 物質P誘發之人類星細胞瘤細胞中磷酸肌醇之生成也 在,例如,體外被頡頗,致產生一大約InM之IC5。値。一適 合檢測此抑制作用之試驗模式爲,例如,李(C.M· Lee)等人 在 J· Neurochem. 59 (1992) 406 - 414 中描述之試驗模式。 本紙張尺度適用中國國家檩準(CNS ) A4規格(210X297公釐) ITAw. (請先閱讀背面之注意事項再填寫本頁) -8 - 經濟部中央標準局員工消費合作社印製 475930 A7 _B7__ 五、發明説明() 在沙鼠中靜脈注射物質P甲酯造成不正常行爲。此效應 可經口服式(I)化合物而被抑制。使用之試驗方法爲法索特 (A· Vassout)等人於 1990 年在 Worchester, Mass·舉行之 ’’Substance P and Related Peptides: Cellular and Molecular Physiology” 會議中發表之 方法。大約口服Oil毫克/公斤顯示有ED50値。這些數據確 立式(I)化合物治療中樞神經系統病症之優異適宜性。 與目前已知之NK1或物質P頡頗劑比較,新穎化合物有 明顯較高之活性以及實質上較高之化學安定性,例如,對 氧之化學安定性,有提升之結晶性以及改進之口服生物利 用性。 因此,本發明提供之式(I)之物質P頡頗劑非常適合醫療 以上說明之病理徵狀。 本發明特別有關那些式(I)化合物,其中之環A未被取 代或被鹵素單取代及環B未被取代或被1-2個由低級院基、 經基、低級院氧基、低級院硫基、鹵素、硝基兒 从執基組成 之一組中選出之取代基取代,以及有關其醫藥上可接與 〇 本發明主要有關那些式(I)化合物,其中之 ^A未被取 代或被氯基單取代及環B未被取代或被1-2個由激# M闲殘基、低級 院氧基'氯基及溴基組成之一組中選出之取代基 及有關其醫藥上可接受之鹽。 代,以 本發明特別有關那些式(I)化合物,其中之 凝A未! 代或被氯基單取代及環B未被取代或被氧_成 % 4復基簞取 代’以及有關其醫藥上可接受之鹽。 本紙張尺度適用中國國家檩準(CNS ) A4規格(210X 297公釐) (請先閲讀背面之注意事項再填寫本頁)
475930 A7 B7 五 發明説明() 要強調之式(I)化合物組之次組各爲:⑻式①化合物, 其中之環A未被取代或在4_位被氯基取代;(b)式①化合物, 其中之環A在位被氯基取代:⑹式①化合物,其中之環b 被氯基或氟基單取代;(d)式(I)化合物,其中之環B未被取 代。 本發明特別有關實施例中描述之特定化合物及其鹽, 特別是其醫藥上可接受之鹽。 式φ化合物可利用本質上已知之方法製備,典型上爲 a)將一式(Ha)化合物 Ο
(Ha) (式(Ila)中之環A及B如式(I)之定義)輿一式(IIb)化合物 -----------噃-------^1-----0 (請先閱讀背面之注意事項再填寫本頁} 經濟部中央標準局員工消費合作社印製
(lib) (式(lib)中之Qi爲可被醚化之羥基,例如’經基、低級院氧 基或未被職之雜職之雜基與反應性酯化經基 (例如鹵素,較適宜者爲氯基)或一下式之自由基 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐)_ 〇 _ 475930 A7 B7 五、發明説明( η
或與其鹽反應;或 b)將一式(Ilia)化合物 f3c
(Ilia) (式(Ilia)中之環A如式(I)之定義)與一式(Illb)化合物 〇
(Illb) (式(Illb)中之環B如式(I)之定義,及Q1爲可被醚化之羥 基,例如羥基、低級烷氧基或未被取代之或被取代之苯氧 基)或與反應性酯化羥基(例如鹵素,較適宜者爲氯基) 經濟部中央標準局員工消費合作社印製 (請先閲讀背面之注意事項再填寫本頁) 或一下式之自由基 〇
或與其鹽反應; 本紙張尺度適用中國國家標準(CNS ) A4規格(210X 297公釐) -11 - 475930 經濟部中央標準局員工消費合作社印製 A7 B7 五、發明説明() 及’需要時,將一式①之化合物轉化成另一式(I)之化合物 及/或’需要時,將得到之鹽轉化成自由化合物或另一鹽 及/或’需要時,將得到之有成鹽性質之式(I)之自由化合 物轉化成鹽及/或,需要時,將得到之一立體異構物或非 鏡像異構物之混合物分離成各個立體異構物及非鏡像異構 物。 含至少一鹼性中心之起始原料之鹽(如那些式(Ila)或 (nia)者)爲相當之酸加成鹽,而含一酸基之起始原料之鹽 (如那些式(lib)或(Illb)者)爲與鹼生成之鹽。 在以下之方法詳述中,除非另有敘述,否則環A及B各 有式(I)之定義。 在上文及下文之方法中描述之反應係利用本質上已知 之方法進行,典型上不使用或,通常,使用適合之溶劑或 稀釋劑或其混合物及,視需求而定,在冷卻、室溫或加熱 下進行,典型上在從大約_8(TC至反應介質之沸騰溫度,較 適宜者爲從大約-10°至大約+200°C之溫度範圍下及,需要 時’在一密封容器內,在壓力下,在一惰性氣壓中及/或 在無水狀態下進行。 另外方法a)及b):製備各個醯胺鍵之縮合反應可利用本質上 已知之方法進行,如在標準著作像”Houben-Weyl,Methodender organischen Chemie",4th dition,Vbl. 15/11,Georg Thieme Veriag,Stuttgart 1974, "The peptides”(ed· E. Gross and J· Meienhofer),Vol· 1 and 2, Academic Press,London and New Υ〇Γ]ς 1979/1980,或 M· Bodanszky,"Principles of Peptide Synthesis”,Springer-Verlag,Berlin 1984 中描述之方法。 本紙張尺度適用中國國家標準(CNS ) A4規格(21〇X297公釐) (請先閲讀背面之注意事項再填寫本頁)
-12- 經濟部中央標準局員工消費合作社印製 475930 A7 B7 五、發明説明() 縮合反應可使用一慣用縮合劑進行。慣用縮合劑典型 上爲羰二亞胺(例如二乙羰二亞胺、二丙羰二亞胺、N-乙-N’-(3_:甲胺丙)簾二亞胺或較適宜者爲二環己羰二亞胺)以 • 及適合之羰基化合物,典型上爲羰二咪唑、1,2-〇§銼化合 物,典型上爲3’_磺酸2-乙_5-苯-1,2-噚銼及過氯酸2-第三丁-5·甲 異嗶銼,或適當之醯胺基化合物,典型上爲2-乙氧-1-乙氧羰-1>二氫喹啉,以及活化之磷酸衍生物,典型上爲二苯磷醯 疊氮、二乙磷醯氰、苯苯磷醯胺氯酸酯、氯化雙(2-氧-3-噚 唑陡)膦酸或六氟磷酸1-苯幷三唑氧叁(二甲胺)錢。 需要時,加入一有機鹼,像含大體積自由基之三低級 烷胺,例如乙二異丙胺,或雜環鹼,典型上爲吡啶、4-二甲 胺吡啶或較適宜者爲N-甲嗎啉。 鹵化醯基,例如,與相當之胺之縮合反應亦可在一適 合之鹼存在下進行,而不需加入適合之耦合成份。 縮合反應宜在一惰性極性非質子性溶劑,最好是無水 溶劑或溶劑混合物中進行,典型上在一羧醯胺(例如甲醯 胺或二甲基甲醯胺)、鹵化烴(例如二氯甲烷、四氯化碳 或氯化苯)、酮(例如丙酮)、環醚(例如四氫呋喃)、 酯(例如醋酸乙酯)或腈(例如乙腈)或其混合物中,在 低或高溫下,典型上在一大約-40°C至大約+100°C,較適宜者 爲大約-l〇°C至大約+50°C之溫度範圍內及,選擇性地,在一 情性氣體壓力下,例如在氮氣下進行。 反應性酸衍生物亦可在在原處生成。 本紙張尺度適用中國國家標準(CNS ) A4規格(210X 297公釐) (請先閲讀背面之注意事項再填寫本頁)
-13- 475930 A7 B7 五、發明説明() 式(lib)及(mb)之起始原料爲已知的,或可利用本質上已 知之方法製備。 式(Ilia)化合物可利用本質上已知之方法製備,而以, 例如式(IIIc)化合物爲起始原料,
(IIIc), 式(fflc)中之Q3爲低級烷基或苯-低級烷基。此化合物典型上 在一鹼存在下,與低級烷氧鹵甲烷(像乙氧氯甲烷)反應 而N-烷化。將形成之式(Hid)化合物
_) (式(md)中之q4爲例如低級烷基),在一強酸(典型上爲 氯磺酸)存在下,用一腈(典型上爲乙腌)處理。將形成 之式(Ille)化合物中之-C(=0)-0Q3基用一強酸(典型上爲氫溴 酸)處理去除, (請先閲讀背面之注意事項再填寫本頁) 、1Τ 經濟部中央標準局員工消費合作社印製 Ο η
(Hie)。 爲了製備鏡像異構純化合物,將如是得到之式(IIIf)化 合物中之第二胺基, 本紙張尺度適用中國國家標準(CNS ) Α4規格(21〇X297公釐) -14- 475930 A7 B7 經濟部中央標準局員工消費合作社印製 五、發明説明( 〇
(Illf), 用一光學活性化合物(典型上爲相當之0-醯化之α-羥羧酸或 其反應性衍生物,例如0-乙醯-(+)苯乙醇醯氯)醯化,及將 如是得到之非鏡像異構物利用本質上已知之方法分離,例 如利用層析術。在去除兩個Ν-醯基後,得到式(fflg)化合物 HN
CH, (nig) 典型上利用酸水解(例如用鹽酸)。將式(Illg)化合物中之4-胺基利用本質上已知之方法暫時保護,典型上係與苯甲醛 反應。然後與一式(lib)化合物耦合,將3,5-雙三氟甲苄醯基 引入,如另外方法a)中所述,然後將保護基去除,典型上 用一酸(像鹽酸)處理,形成一相當之式(Ilia)化合物。 式(Ila)化合物可利用本質上已知之方法製備,典型上以 一式(Illg)化合物爲起始原料,將其在一耦合劑存在下與一 式(Illb)化合物耦合,如另外方法b)中所述,因此引入相當 之醯基。如是得到相當之式(Ila)化合物。 得到之鹽可利用本質上已知之方法轉化成自由化合 物,典型上用鹼處理,例如用鹼金屬氫氧化物、金屬碳酸 鹽或碳酸氫鹽、或最初提到之另一成鹽鹼處理,或用酸處 本紙張尺度適用中國國家標準(CNS ) Α4規格(210X 297公釐) ----------II (請先閲讀背面之注意事項再填寫本頁) 、1Τ -15- 475930 A7 B7 五、發明説明() 理,典型上用礦物酸(像氯化氫)或開始時提到之另一成 鹽酸處理。 得到之鹽可利用本質上已知之方法轉化成其它鹽,在 酸加成鹽之情況,典型上在一適當溶劑中(形成之無機鹽 不溶於其中,因而可從反應平衡中消除者),用另一酸之 適當金屬鹽(像鈉鹽、鋇鹽或銀鹽)處理,及在鹼性鹽之 情況,係利用形成自由酸及重覆鹽生成。 式(I)化合物(包括其鹽)亦可以水合物形式得到,或 也可包含結晶時使用之溶劑。 由於新穎化合物之自由形式與其鹽形式間之緊密關 係,在說明書中述及之自由化合物及其鹽亦類推地適用於 相當之鹽或自由化合物。 由於其成份間之物理化學差異,得到之非鏡像異構物 及消旋物混合物可利用已知方法分離成純非鏡像異構物及 消旋物,典型上利用層析術及/或分段結晶。 經濟部中央標準局員工消費合作社印製 (請先閲讀背面之注意事項再填寫本頁) 形成之消旋物可利用已知方法進一步分離成光學對映 體,典型上是用從一光學活性溶劑中再結晶,使用微生物 或將形成之非鏡像異構混合物或消旋物與一光學活性輔助 化合物反應,例如,視式(I)化合物中存在之酸基、鹼基或 官能可修飾基而定,與一光學活性酸、鹸或與光學活性醇 反應,形成非鏡像異構鹽及官能衍生物(像酯)之混合 物,將其分離成非鏡像異構物,從其中可利用各別常用方 法釋出各別希望之鏡像異構物。適合此目的之鹼、酸及醇 典型上爲光學活性蠄鹼,像番木鼈雉、辛可寧或百路新、 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) -16 - 475930 A7 B7______ 五、發明説明() 或D-或L-(l-苯)乙胺、3_甲六氫吡啶、麻黃蠄、安非他命及 合成得到之類似鹼、光學活性羧酸或磺酸’像金雞鈉酸或 D_或L_酒石酸、D-或L·二-鄰甲苯酒石酸、D·或L-蘋果酸、D-或L-苯乙醇酸或D-或L-樟腦磺酸、或光學活性醇,像萡醇 或D-或L-(l-苯)乙醇。 本發明亦有關此方法之那些具體實施例’其中在方法 之任何階段得到爲中間體之化合物可用作起始原料並進行 其餘步驟,或起始原料以鹽形式使用或,最好是,在反應 條件下生成。 本發明亦有關製備新穎化合物而特別發展之新穎起始 原料,特別是那些形成最初描述之特別偏愛之式(I)化合物 之起始原料,有關其製備方法及其作爲中間體之用途。 經濟部中央標準局員工消費合作社印製 (請先閲讀背面之注意事項再填寫本頁) 新穎之式(I)化合物可,例如,以醫藥組成物形式使 用,其含一有效醫療量之有效成份,適當時連同無機或有 機,固體或液體,之適合經腸服用(例如口服)或非經腸 服用之醫藥上可接受之載體。因此,以錠劑或明膠膠囊劑 型使用,其中含有效成份連同稀釋劑,典型上爲乳糖、葡 萄糖、蔗糖、甘露糖醇、葡萄糖醇、纖維素及/或潤滑 劑,例如矽藻土、滑石、硬脂酸或其鹽(像硬脂酸鎂或硬 脂酸鈣)、及/或聚乙二醇。錠劑亦可含結合劑,典型上 爲矽酸鋁鎂、澱粉(典型上爲玉米澱粉、小麥澱粉、米澱 粉或葛澱粉)、明膠、黃耆膠、甲基纖維素、羧甲基纖維 素鈉及/或聚乙烯吡咯酮,及,需要時,含分散劑,典型 上爲澱粉、瓊脂、海藻酸或其鹽(例如海藻酸鈉)、及/ 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) -17- 475930 A7 B7 五、發明説明() (請先閱讀背面之注意事項再填寫本頁) 或發泡混合物、或吸收劑、著色劑、香料及增甜劑。新穎 之式(I)化合物亦可以非經腸服用組成物或輸液溶液形式使 用。此溶液宜爲等滲壓水溶液或懸浮液,例如在單獨含有 效成份或連同一載體(像甘露糖醇)之凍乾組成物之情 況,其可在使用前製備。醫藥組成物可經滅菌處理及/或 可含輔劑,典型上爲防腐劑、安定劑、增濕劑及/或乳化 劑、溶解化劑、調節滲透壓之鹽及/或緩衝劑。如是得到 之醫藥組成物(其,需要時,含另外之藥理活性物質)係 利用本質上已知之方法,用傳統之混合、製粒、塗糖膜、 溶解或冷凍乾燥方法製備,且含大約0.1%至100%,較適宜 者爲大約1%至大約50% (凍乾物至大約100%)之有效成份。 本發明亦有關式(I)化合物之用途,最好是在醫藥組成 物形式。劑量可視各種因素像服用方式、物種、年齡及/ 或個別狀況而定。在口服之情況,每日劑量爲大約0.25至10 毫克/公斤,且對重約70公斤之溫血動物,每日劑量宜爲 大約20毫克至大約500毫克。 本發明係利用以下之實施例說明,其中之溫度單位爲 °C及壓力單位爲毫巴。FD-MS =場脫附質譜術。 經濟部中央標準局員工消費合作社印製 實施例1 : (2民你>沁『1_(3,5-雙三氟甲苄醯)-2-(4-氯苄)六氫吡啶-4- 基H-氧苯幷哌喃-2-羧醯胺 將3.77毫升三乙胺及2.35克4-氧-4H-1-苯幷哌喃-2-羧醯氯 (由相當之羧酸(由,例如,Sigma公司提供)與氯化硫醯 基反應而得)加入一 4.36克(2民48)-4-胺_1·(3,5-雙三氟甲节權)-2- 本紙張尺度適用中國國家標準(CNS ) A4規格(210X 297公釐) -18- 475930 五 經濟部中央標率局員工消費合作社印製 A7 B7 _ 發明説明() (4-氯苄)六氫吡啶溶於200毫升二氯甲烷之溶液中,並在20°C 下,將混合物攪拌4小時。將反應混合物用IN鹽酸水溶液 淸洗,然後用鹽水及水淸洗,經由硫酸鎂乾燥及蒸發濃 縮。將得到之泡沬從第三丁基甲基醚/己烷/二氯甲烷中 結晶,產生無色晶狀之標題化合物,熔點:211-212°。[a]D2() =3.7 ±2.6(c = 0.382,甲醇)。 起始化合物可製備如下: a) 氯苄)丁-3-烯1-N-乙氧甲胺甲酸甲酯:將一 10.0克氫化 鈉(8〇%在礦油中,333毫莫耳)溶於無水四氫呋喃[THF]中 之懸浮液在氬氣下迴流。在1小時內,逐滴加入一 60.5克 (238 毫莫耳)[1-(4-氯苄)丁·3_烯]胺甲酸甲酯[McCarty FJ et al.,J. Med· Chem,1968, 11(3),534]溶於50毫升無水四氫呋喃中之溶 液。然後將混合物迴流2小時直到氣體不再逸出爲止。將混 合物冷卻至〇°C,並逐滴加入氯甲基乙基醚,使反應溫度不 昇高超過5°C。然後將混合物緩緩熱至25°C,並攪拌12小 時。在加入更多水之前,將過量的氫化鈉小心地用1毫升水 破壞。將相分離,並將水相用第三丁基甲基醚萃取。將收 集之有機相用鹽水淸洗,經由硫酸鈉乾燥及蒸發濃縮。將 粗產物在0.1毫巴下蒸餾,並有一 120至125°C之沸點範圍。 DC:醋酸乙酯/ 己烷(l:6)Rf=0.34, FD_MS:M+ = 311(313)。 b) (2R*,4S*)-4-乙醯胺-2_(4-氯f)六氫吡啶-1-羧酸甲酯:在-40。。 下,將20·6克(3Q8毫莫耳)氯磺酸加入500毫升乙勝中。將 一 48.0克(1Μ毫莫耳)Ν-[1·(4-氯苄)丁·3_烯]-Ν-乙氧甲胺甲酸 甲酯溶於50毫升乙腈之溶液逐滴加入此混合物中,使反應 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) (請先閱讀背面之注意事項再填寫本頁)
-19- 475930 A7 B7 五、發明説明() (請先閲讀背面之注意事項再填寫本頁) 溫度不昇高超過-lot:。在-15°C下,將反應混合物攪拌20分 鐘,然後加入370毫升之2N氫氧化鈉溶液及1〇〇毫升之10%碳 酸氫鈉水溶液。將相分離,並將水相用甲苯萃取兩次。將 收集之經由硫酸鈉乾燥。將粗產物從甲苯中結晶,產生白 色晶狀之標題化合物。熔點:169_170°C。DC:二氯甲烷/ 甲醇 / 濃氨(90:9:1) Rf = 0.42,FD-K1S: M+ = 325。 c) (2R*,4S*>N42-(4-氯苄)六氫吡啶-4·基1乙醯胺:將51.8毫升之 33%溴化氫溶於醋酸之溶液加入(2R*,4S*>4-乙醯胺-2-(4-氯节)六 氫吡啶小羧酸甲酯(30.0克,92.3毫莫耳)中。16小時後, 將200毫升水加入混合物中,然後將其用甲苯淸洗兩次。將 水相鹼化,並用醋酸乙酯萃取兩次。將有機相經由鉀乾 燥,並在一旋轉蒸發器內蒸發濃縮。標題化合物以氫氯化 物形式從乙醇/醋酸乙酯中結晶。熔點:288_289°C。DC: 二氯甲烷 / 甲醇 / 濃氨(9〇··9··1) Rf = 0·Π,FD-MS: (M+l)+ = 267。 經濟部中央標準局員工消費合作社印製 d) (2,S,2民4S)醋酸-2-『4-乙醯胺-2-(4-氯节)六氫卩比陡小基氧-1-苯基 乙酯:在0°C及劇烈攬拌下,將消旋之氫氯化Ν-[2-(4-氯苄)六 氫吡啶-4·基]乙醯胺(20.5克,07.6毫莫耳)加入34毫升之2Ν 氫氧化鈉溶液、150毫升之10%碳酸氫鈉水溶液及5〇毫升二 氯甲烷中。在1小時,逐滴加入s(+>〇-乙醯苯乙醇醯氯 [Pracejus G,Ann·,1959, 622, 10] ( 14.9 克,7〇 毫莫耳)。然後在 +4 。(:,將混合物攪拌1小時。將相分離,並將有機相經由硫酸 鈉乾燥,並在一旋轉蒸發器內蒸發濃縮。從二氯甲烷/第 三丁基甲基醚中結晶兩次後,分離出純非鏡像異構物形式 本紙張尺度適用中國國家標準(CNS ) A4規格(21〇X297公釐) 475930 五 經濟部中央標準局員工消費合作社印製 A7 B7 發明説明() 之標題化合物。熔點:209-211°C。DC:二氯甲烷/異丙醇 (9·· 1) Rf = 0.65,FD-MS: M+ = 443。[ocf = +77.5。(c=l,二氯甲烷)。 母液主要含非晶狀非鏡像異構物(2’S,2S,4R)-N-[2-(4-氯苄)-1-(乙醯氧苯乙醯)六氫吡啶-4-基]乙醯胺,DC:二氯甲烷/異丙 醇(9:l)Rf=0.70。 e) (gR^SM-胺小(3,5-雙三氟甲苄醯),2·(4-氯苄)六氣吡啶:將 (2’S,2IMS)醋酸-2·[4-乙醯胺_2-(4_氯f)六氫吡陡小基]_2·氧·ι·苯基乙 酯(37.4克,84.5毫莫耳)在370毫升之6N鹽酸中迴流2天。 冷卻後,將混合物用固體氫氧化鈉鹼化,並用二氯甲烷萃 取。將收集之有機相經由碳酸鉀乾燥,並在一旋轉蒸發器 內蒸發濃縮。將含幾乎純(2民48>2-(4_氯)六氫吡啶-4-胺(19.0 克,84.5毫莫耳,100%)之剩餘物溶入8.5毫升(84.5毫莫 耳)苯甲醛中,並在一旋轉蒸發器內,用150毫升甲苯濃縮 兩次。將油狀剩餘物溶入180毫升二氯甲烷及15.3毫升(110 毫莫耳)三乙胺中,並冷卻至l〇°C。在15分鐘內,逐滴加 入雙三氟甲苄醯氯(25.7克,92·9毫莫耳),然後在25°C 下,將混合物攪拌1小時。將250毫升之IN鹽酸加入反應混 合物中,並在一旋轉蒸發器內,將二氯甲烷在減壓下去 除。加入己烷及乙醇直到得到兩個均勻相爲止。將有機相 去除,並將混合物用己烷淸洗直到苯甲醛完全去除爲止。 將混合物用固體氫氧化鈉鹼化,並用氫氧化鈉溶液重覆萃 取。將有機相經由硫酸鈉乾燥,並在一旋轉蒸發器內濃 縮。從第三丁基甲基醚/己烷中結晶,產生白色晶狀之標 題化合物。熔點:79-81°C。DC:二氯甲烷/甲醇/濃氨 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) (請先閱讀背面之注意事項再填寫本頁) -21 - 經濟部中央標準局員工消費合作社印製 475930 Α7 Β7 五、發明説明() (90:9:1) Rf= 0.21。FD_MS: (M+l)+ = 465。[ocf = -12.7° (c二1,二氯甲 烷)。 以下之化合物亦可依照實施例1中描述之一般程序製 備。相當之起始原料(2民4S)-4-胺-l-(3,5-雙三氟甲苄醯)-2·苄六 氫吡啶之製備係描述在專利案EP-A-532456之實施例38f中: 實施例1/1 : (2民4S)-N-[1_(3,5-雙三氟甲苄醯>2-苄六氫吡啶斗基]-4_氧 _4Η·1·苯幷哌喃-2-羧醯胺,熔點:107 - 108°,[oc]D2G=18.3 士 2.6 (c=0.388,甲醇) 實施例1/2 : (2化48)_仏[1-(3,5_雙三氟甲苄醯)_2_f六氫吡啶-4-基]-7-氯_4·氧_4H-1-苯丼哌喃-2_殘醯胺,熔點:224-:226°,[oc]d2() = 21.5 ± 2.5 (c二0.40,甲醇 > 實施例1/3 : (2民48>乂[1-(3,5-雙三氟甲苄醯>2-苄六氫吡啶斗基]-7·甲氧—4-氧苯幷哌喃-2-羧醯胺,熔點:190- 192。,[a]D20 = 25·7 ± 2·3 (c=0.44,甲醇) 實施例1/4 : (2民4S)_N-[l-(3,5-雙三氟甲苄醯)_2·苄六氫吡啶-4-基]-7_甲硫-4_氧·4Η-1-苯幷哌喃-2_羧醯胺 實施例1/5 : (2民4S)-N-[l-(3,5·雙三氟甲苄醯)-2-苄六氫吡啶-4_基]- 6_甲氧-4-氧苯幷峨喃-2-竣釀胺 實施例1/6 : (2艮4S)-N-[l-(3,5-雙三氟甲苄醯>2-苄六氫吡啶_4_基]-6·氯斗氧-4Η_1·苯幷哌喃_2_羧醯胺 實施例1/7 : (2民4S)-N-[1_(3,5-雙三氟甲苄醯)_2_苄六氫吡啶-4-基]-6-溴-4-氧-4H-1-苯幷哌喃-2-羧醯胺 實施例1/8 : (2Κ4δ>Ν·[1·(3,5-雙三氟甲苄醯)-2-节六氫吡啶_4_基]-6·氟·4_氧_4H小苯幷哌喃·2_殘醯胺 本紙張尺度適用中國國家標準(CNS ) Α4規格(210X 297公釐) (請先閲讀背面之注意事項再填寫本頁)
-22- 475930 Α7 Β7 五、發明説明() 實施例1/9 : (2民4S>N-[l-(3,5-雙三氟甲苄醯)-2-苄六氫吡啶-4-¾-6_甲_4·氧-4H-1-苯幷哌喃·2·羧醯胺 實施例m〇 : (2艮48)_乂[1-(3,5·雙三氟甲苄醯)-2-苄六氫吡啶-4-基]-6-氰-4-氧-4H-1-苯幷哌喃-2-羧福胺 實施例1/11 : (211^)-1^1-(3,5-雙三氟甲苄醯)-2-苄六氫吡啶-4-基]- 6- 硝-4·氧-4H小苯幷哌喃_2_羧醯胺 實施例1八2 : (2民4S)-N-[l-(3,5_雙三氟甲苄醯)-2_苄六氫吡啶斗基]- 7- 氟-4·氧-4H-1-苯幷哌喃-2-羧醯胺 實施例U13 : (2R^S)-N-[1_(3,5-雙三氟甲苄醯)-2-苄六氫吡啶-4-基]-7-溴-4-氧-4H-1-苯幷哌喃-2-羧醯胺 實施例1/14 : (2R^4S)_N_[l-(3,5_雙三氟甲苄醯)_2_苄六氫吡啶斗基]-7_甲_4_氧4Η·1_苯幷哌喃-2_竣醯胺 實施例t/15 : (2IMS)-N-[1_(3,5-雙三氟甲苄醯>2-苄六氫吡啶斗基]-7-硝-4-氧-4H-1-苯幷哌喃-2-羧醯胺 實施例1/16 : (2Κ^>·Ν-[1-(3,5·雙三氟甲苄醯)-2-苄六氫吡啶斗基]· 6,7-二甲氧冰氧·4Η小苯幷嘁喃-2·竣醯胺。 經濟部中央標準局員工消費合作社印製 (請先閱讀背面之注意事項再填寫本頁) 實施例2 : (2IUSVN4H3,5-雙三氟甲苄醯)-2-苄六氫吡啶-4·基1-7-羥_4_氧_4H小苯幷哌喃-2-羧醯胺 將一 0·127克(2民4S)本胺小(3,5-雙三氟甲苄醯)-2-苄六氫吡 啶溶於3.1毫升二氯甲烷之溶液溶入0.038克4-二甲胺吡啶、 0.059克氣氯化N-(3-二甲胺丙)-Ν’-乙-幾二醯亞胺及〇·〇64克7-羥-4-氧-4Η-1-苯幷_喃羧酸溶於2毫升二氯甲烷/二甲基甲醯胺 (1:1)之溶液中,並在20°下攪拌24小時。將反應混合物蒸發 本紙張尺度適用中國國家標準(CNS ) Α4規格(210X 297公釐) -23- 475930 A7 B7 五、發明説明() 濃縮,並將剩餘物在矽膠上,用二氯甲烷及二氯甲烷/甲 醇(19:1)層析,產生淡黃色粉末狀之標題化合物,熔點:224-225° ; [gc]d20 = 235 ± 3.5 (c=0.288,甲醇)。 以下之化合物亦可依照實施例2中描述之一般程序製 備· 實施例2/1 ·· (2IMS)-N-[K3,5-雙三氟甲苄醯)·2-节六氫吡啶斗 6-溴-7_羥-4_氧-4Η小苯幷哌喃-2-羧醯胺。熔點:173- 174° 實施例3 :以下之化合物亦可依照實施例1中描述之一般程 序製備,而以(2民4S>4-胺-1-(3,5-雙三氟甲苄醯)-2-(4-氯苄)六氫 吡啶〔實施例le)〕爲起始原料: 實施例3/1 : (2民48)善[1_(3,5-雙三氟甲苄醯)-2·(4-氯苄)六氫吡啶· 4-基]-7_氯-4-氧-4Η-1·苯幷哌喃-2-羧醯胺。熔點:218-220。,[0¾20 = 31.5±2.0(c=0.50,甲醇) 實施例3/2 : (2氏48)1[1-(3,5-雙三氟甲苄醯)-2-(4-氯节)六氫吡陡_ 4-基]-7-甲氧-4-氧-4H-1-苯幷峨喃-2-竣醯胺。溶點:198 - 200°, [oc]D20 = 29·7 土 2·2 (c=0.45,甲醇) 經濟部中央標準局員工消費合作社印製 (請先閱讀背面之注意事項再填寫本頁) 鬣施例3/3 : (2R^S)-N-[K3,5-雙三氟甲苄醯)-2-(4-氯f)六氫吡陡· 4-基]-7-甲硫-4-氧-4H-1-苯幷哌喃-2-羧醯胺。熔點:137 - 140°, [a]D20 = 20.8 土 2.8 (c=0.355,甲醇) 宣施例说·· (2艮4S)_N-[l_a5-雙三氟甲苄醯)-2_(4-氯苄)六氫吡啶-4-基]-6-甲氧-4-氧-4H-1-苯幷哌喃·2·竣醯胺 &適例3/5 ·· (2MS)-N-[l-(3,5-雙三氟甲苄醯)-2-(4-氯苄)六氫吡啶-4-基]_6·氯_4-氧_411-1_苯幷峨喃-2-竣釀胺 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) -24- 五 經濟部中央標準局員工消費合作社印製 475930 A7 B7 發明説明() 實施例3/6 : (21^48)-化[1_(3,5_雙三氟甲苄醯)-2-(4-氯节)六氫吡陡-4-基溴-4-氧-4H-1-苯幷哌喃-2-羧醯胺 實施例3/7 : (2民4S)-N-[1_(3,5·雙三氟甲苄醯)冬(4·氯f)六氫吡陡-4-基]-6-氟-4-氧-4H-1-苯幷哌喃-2-羧醯胺。熔點:215-218°; Rf(醋 酸乙酯/己烷4:1) =Ό.58。所需之起始原料醯氯6-氟-4-氧-4H-1-苯幷峨喃-2_竣釀氯特別描述在Chemical Abstracts: 96:52132w或 88:106066w 中,並有CAS 登錄號65843·87·0。 實施例3/8 : (2R,4S)-N-[l-(3,5_雙三氟甲苄醯)-2-(4-氯f)六氫吡陡· 4-基]_6_甲氧苯幷哌喃竣醯胺。熔點:240-241°; Rf(醋 酸乙酯/己烷4:1) = 0.65。 實施例3/9 ·· (2R^S)-N-[l-(3,5·雙三氟甲苄醯)-2-(4-氯节)六氫吡陡· 4·基氰-4·氧-4H-1-苯幷哌喃-2-羧醯胺。 實施例3/10 : (2民4S)_N_[l-(3,5_雙三氟甲苄醯)_2·(4_氯f)六氫吡啶 基]-6-硝4-氧-4H-1-苯幷哌喃-2-羧醯胺。 實施例3/11 ·· (2氏48)-仏[1-(3,5_雙三氟甲苄醯)-2-(4-氯节)六氫吡啶 4-基K7-氟氧4Η-1-苯幷哌喃-2-羧醯胺。 實施例3Α2 : (2IUS)-N-[l-(3,5-雙三氟甲苄醯)-2-(4-氯节)六氫吡啶 -4·基]-7·溴-4-氧《4Η-1-苯幷峨喃-2-錢醯胺。 實施例3/13 : (m^SKHK3,5-雙三氟甲苄醯)-2-(4-氯f)六氫吡啶 斗基]甲斗氧-4Η-1·苯幷哌喃_2·羧醯胺。 實施例3/14 : (2艮48)1[1-(3,5_雙三氟甲苄醯)-2-(4-氯f)六氫吡啶 •4-基]-7·5肖-4·氧-4H-1-苯幷哌喃-2·羧醯胺。 實施例3/15 : (2民4S)-N-[l-(3,5-雙三氟甲苄醯)冬(4-氯苄)六氫吡啶 冬基]-6,7-二甲氧_4-氧_411_1-苯幷哌喃-2·錢醯胺。 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) (請先閲讀背面之注意事項再填寫本頁)
25- 475930 A7 B7 ^___ 經濟部中央標準局員工消費合作社印製 發明説明() 實施例4 :含50毫克有效成份之錠劑可製備如下: 組成(10000顆錠劑) (請先閲讀背面之注意事項再填寫本頁) 有效成份 500.0克 乳糖 500.0克 馬鈴薯澱粉 352.0克 明膠 8.0克 滑石 60.0克 硬脂酸鎂 1〇.〇克 二氧化矽(高分散性) 20·0克 乙醇 適量 將有效成份與乳糖及292克馬鈴薯澱粉混合,然後將混 合物用一明膠乙醇溶液潤濕,並經由篩製粒。乾燥後,摻 入其餘之馬鈴薯澱粉、硬脂酸鎂、滑石及二氧化矽,並將 混合物壓成錠劑,各重145.0毫克及含50.0毫克有效成份。需 要時,錠劑可具有分裂凹痕以爲更細之劑量調配。 實施例5 :含100毫克有效成份之膜衣錠可製備如下: 組成(1000顆膜衣錠) 有效成份 100.0克 乳糖 100.0克 玉米澱粉 70.0克 滑石 8.5克 硬脂酸鈣 1.5克 羥丙基甲基纖維素 2.36克 蟲膠 0.64克 水 適量 二氯甲烷 適量 本紙張尺度適用中國國家標準(CNS ) Α4規格(210X297公釐) -26- 475930 經濟部中央標準局員工消費合作社印製 A7 B7 五、發明説明() 將有效成份、乳糖及40克玉米澱粉混合,並用一由15 克玉米澱粉及水(在加熱下)製備之糊劑潤濕及製粒。將 顆粒乾燥,並加入其餘之玉米澱粉、滑石及硬脂酸鈣,並 與顆粒混合。將混合物壓成錠劑(重2S0毫克),然後將其 用一羥丙基甲基纖維素及蟲膠溶於二氯甲烷之溶液塗膜。 膜衣錠之最後重量爲283毫克。 竇施例6 :含100毫克有效成份之明膠乾充塡膠囊可,例 如,製備如下: 組成(1000顆膠囊) 有效成份 100.0克 乳糖 250.0克 微晶纖維素 30.0克 硫酸月桂酯鈉 2.0克 硬脂酸鎂 8.0克 將硫酸月桂酯鈉通過一 0.2毫米網目大小之篩加入凍乾 之有效成份中。將兩成份緊密混合。接著先將乳糖篩過一 0.6毫米網目大小之篩加入,然後將微晶纖維素篩過一 0.9毫 米網目大小之篩加入。將混合物再次緊密混合1〇分鐘。最 後將硬脂酸鎂篩過一 0.8毫米網目大小之篩加入。再混合3 分鐘後,將每一 390毫克如是得到之組成物塡入〇號明膠乾 充塡膠囊中。 實施例7 :含0.1% (重量百分比)有效成份之含推進劑之吸 劑懸浮液: (請先閱讀背面之注意事項再填寫本頁) 、τ 本紙張尺度適用中國國家標準(CNS ) A4規格(210X297公釐) 475930 Α7 Β7 五、發明説明() 組成 %(重量百分比) 微粒化有效成份 0.1 三油酸葡萄聚糖酯 0.5 推進劑A(三氯三氟乙烷) 4.4 推進劑B (二氯二氟甲烷及 15.0 1,2-二氯四氟乙烷) 80.0 使用一傳統均質機,在排除水份下,加入Η油酸葡萄 聚糖酯,將有效成份懸浮在三氯三氟乙烷中,然後將懸浮 液塡入一備有劑量控制閥之劑氣溶膠容器內。將容器密 封,並加壓塡入推進劑Β。 (請先閱讀背面之注意事項再填寫本頁) #本· I.訂 經濟部中央標準局員工消費合作社印製 本紙張尺度適用中國國家標準(CNS ) Α4規格(210X 297公釐) -28-
Claims (1)
- 475930 A B c D 第85104270號專利申請案 中文申請專利範圍修正本(90年11月) 六、申《請專利範圍其中環A未被取代或被南素單取代,環b未被取代或被 1 -2個選自由C丨-4低級烷基、羥基、c卜4低級烷氧 基、C 1 -4低級烷硫基及卣素所組成之群之取代基取 代,或其醫藥上可接受之鹽。 2 ·如申請專利範圍第1項之式(〗)化合物,其中之環A未被 取代或被氯單取代,環B未被取代或被1 _ 2個選自由輕 基、C丨-4低級烷氧基、氯及溴所組成之群之取代基取 代,或其醫藥上可接受之鹽。 3 ·如申請專利範圍第1項之式(〗)化合物,其中之環a未被 取代或被氯單取代,環B未被取代或被氯或氟取代,或 其醫藥上可接受之鹽。 4 ·如申請專利範圍第1項之式(〗)化合物,其中式(〗)化合 物為式(I a)之非鏡像異構形式: O:\56\56552DOC 本紙張尺度適用中國國家標準(CNS) A4規格(210 X 297公爱) A8 B8 C8 D8 申请專利範圍5·如申請專利範圍第1項之式(I)化合物,其係(2R , 4S)-N-[l-(3 , 5_雙三氟甲芊醯基)·2_(4_氯苄基)六 氫吡哫·4_基]氧·4Η-1-苯并哌喃-2-羧醯胺或其醫 藥上可接受之鹽。 、 6·如申請專利範圍第1項之式(I)化合物,其係(2 R , 4S)-N-[l-(3,5_雙三氟甲基芊醯基)·2·芊六氫吡啶_ 4 -基]-4 -氧- 4Η-1-苯并哌喃-2-羧醯胺或其醫藥上可 接受之鹽。 7·如申請專利範圍第1項之式(I)化合物,其係(2 R, 4S)-N-[l-(3,5·雙三氟甲基苄醯基)_2_(4-氯苄基) 穴虱吡啶基]·6_氟-4-氧-4H-1-苯并哌喃-2·羧醯 胺或其醫藥上可接受之鹽。 8· —種用於治療對頡頑神經激肽1(ΝΚ1)受體起反應之疾 病 < 醫藥組成物,其含申請專利範圍第b 7項中任一項 之化合物及至少一種醫藥上可接受之載體。 9·如申請專利範圍第1β7項中任一項之化合物,其係用於 -2 O:\56\56552.DOC 本纸張尺度適用中國國家標準(CNS) Α4規格(210X297公釐) 475930 申請專利範圍 8 8 8 8 A B c D 治療對頡頑神經激肽1 (ΝΚ 1 )受體起反應之疾病 O:\56\56552.DOC本纸張尺度適用中國國家標準(CNS) A4規格(210 X 297公釐)
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| EP (1) | EP0739892B1 (zh) |
| JP (1) | JP3068458B2 (zh) |
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| CN (1) | CN1063176C (zh) |
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| AT (1) | ATE224891T1 (zh) |
| AU (1) | AU714523B2 (zh) |
| BR (1) | BR9602025A (zh) |
| CA (1) | CA2174707C (zh) |
| DE (1) | DE59609707D1 (zh) |
| DK (1) | DK0739892T3 (zh) |
| ES (1) | ES2183923T3 (zh) |
| HU (1) | HUP9601062A3 (zh) |
| IL (1) | IL117989A (zh) |
| NO (1) | NO309813B1 (zh) |
| NZ (1) | NZ286422A (zh) |
| PT (1) | PT739892E (zh) |
| RU (1) | RU2156250C2 (zh) |
| TW (1) | TW475930B (zh) |
| ZA (1) | ZA963211B (zh) |
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| WO1997044035A1 (en) * | 1996-05-24 | 1997-11-27 | Eli Lilly And Company | Methods of treating hypertension |
| TW426667B (en) * | 1997-11-19 | 2001-03-21 | Pfizer | Piperidinylaminomethyl trifluoromethyl cyclic ether compounds as substance P antagonists |
| BR9913201A (pt) * | 1998-08-25 | 2001-05-08 | Novartis Ag | Uso de antagonista da substância p para o tratamento da sìndrome da fadiga crÈnica e/ou fibromialgia e uso de antagonistas do recptor de nk-1 para tratamento da sìndrome da fadiga crÈnica |
| DE60001736T2 (de) * | 1999-05-21 | 2003-09-18 | Pfizer Prod Inc | 1-trifluorotmethyl-4-hydroxy-7-piperidinyl-aminomethylchroman-derivate |
| GB0220953D0 (en) * | 2002-09-10 | 2002-10-23 | Novartis Ag | Organic compounds |
| GB2394417A (en) * | 2002-10-24 | 2004-04-28 | Novartis Ag | Solid dispersion comprising a piperidine substance P antagonist and a carrier |
| DE10256174A1 (de) * | 2002-12-02 | 2004-06-09 | Merck Patent Gmbh | 2-Benzoylchromonderivate |
| DE10256182A1 (de) * | 2002-12-02 | 2004-06-24 | Merck Patent Gmbh | 2-Oxadiazolchromonderivate |
| US20050209274A1 (en) * | 2004-02-26 | 2005-09-22 | Lynch John K | Antagonists of melanin concentrating hormone effects on the melanin concentrating hormone receptor |
| CN1300163C (zh) * | 2004-06-23 | 2007-02-14 | 南京大学 | 3-羟基色原酮糖苷及其制法和用途 |
| JP2009534399A (ja) * | 2006-04-18 | 2009-09-24 | アボット・ラボラトリーズ | バニロイド受容体サブタイプ1型(vr1)の拮抗薬およびその使用 |
| GB0701365D0 (en) * | 2007-01-24 | 2007-03-07 | Glaxo Group Ltd | Novel pharmaceutical compositions |
| UA105182C2 (ru) | 2008-07-03 | 2014-04-25 | Ньюрексон, Інк. | Бензоксазины, бензотиазины и родственные соединения, которые имеют ингибирующую nos активность |
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| DE3117389A1 (de) * | 1981-05-02 | 1982-11-18 | Boehringer Mannheim Gmbh, 6800 Mannheim | Benzopyranylether, verfahren zu deren herstellung sowie diese verbindungen enthaltende arzneimittel |
| MY110227A (en) * | 1991-08-12 | 1998-03-31 | Ciba Geigy Ag | 1-acylpiperindine compounds. |
| AU7856194A (en) * | 1993-10-26 | 1995-05-22 | Ciba-Geigy Ag | N-benzoyl-4-oxy/thio-2-substituted piperidines as substance-p receptor antagonists |
| ES2172595T3 (es) * | 1994-09-30 | 2002-10-01 | Novartis Ag | Compuestos de 1-acil-4-alifatilaminopiperidina. |
| TW397825B (en) * | 1994-10-14 | 2000-07-11 | Novartis Ag | Aroyl-piperidine derivatives |
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1996
- 1996-04-11 TW TW085104270A patent/TW475930B/zh not_active IP Right Cessation
- 1996-04-11 RU RU96107121/04A patent/RU2156250C2/ru not_active IP Right Cessation
- 1996-04-16 DE DE59609707T patent/DE59609707D1/de not_active Expired - Lifetime
- 1996-04-16 DK DK96810237T patent/DK0739892T3/da active
- 1996-04-16 PT PT96810237T patent/PT739892E/pt unknown
- 1996-04-16 AT AT96810237T patent/ATE224891T1/de not_active IP Right Cessation
- 1996-04-16 US US08/632,971 patent/US5604247A/en not_active Expired - Lifetime
- 1996-04-16 ES ES96810237T patent/ES2183923T3/es not_active Expired - Lifetime
- 1996-04-16 EP EP96810237A patent/EP0739892B1/de not_active Expired - Lifetime
- 1996-04-21 IL IL11798996A patent/IL117989A/xx active IP Right Grant
- 1996-04-22 NZ NZ286422A patent/NZ286422A/en unknown
- 1996-04-22 CA CA002174707A patent/CA2174707C/en not_active Expired - Fee Related
- 1996-04-22 AU AU50805/96A patent/AU714523B2/en not_active Ceased
- 1996-04-23 JP JP8101568A patent/JP3068458B2/ja not_active Expired - Fee Related
- 1996-04-23 CN CN96106111A patent/CN1063176C/zh not_active Expired - Fee Related
- 1996-04-23 ZA ZA963211A patent/ZA963211B/xx unknown
- 1996-04-23 HU HU9601062A patent/HUP9601062A3/hu unknown
- 1996-04-23 KR KR1019960012355A patent/KR100416674B1/ko not_active IP Right Cessation
- 1996-04-23 NO NO961616A patent/NO309813B1/no unknown
- 1996-04-24 BR BR9602025A patent/BR9602025A/pt not_active IP Right Cessation
- 1996-04-24 AR AR33626596A patent/AR001813A1/es unknown
Also Published As
| Publication number | Publication date |
|---|---|
| HUP9601062A2 (en) | 1997-10-28 |
| NZ286422A (en) | 1998-01-26 |
| AU714523B2 (en) | 2000-01-06 |
| NO961616L (no) | 1996-10-25 |
| NO961616D0 (no) | 1996-04-23 |
| AR001813A1 (es) | 1997-12-10 |
| IL117989A0 (en) | 1996-08-04 |
| JPH093066A (ja) | 1997-01-07 |
| JP3068458B2 (ja) | 2000-07-24 |
| NO309813B1 (no) | 2001-04-02 |
| US5604247A (en) | 1997-02-18 |
| MX9601515A (es) | 1997-09-30 |
| ATE224891T1 (de) | 2002-10-15 |
| HUP9601062A3 (en) | 1998-10-28 |
| BR9602025A (pt) | 1998-10-06 |
| HU9601062D0 (en) | 1996-06-28 |
| CN1141921A (zh) | 1997-02-05 |
| ZA963211B (en) | 1996-10-24 |
| DK0739892T3 (da) | 2003-01-20 |
| PT739892E (pt) | 2003-01-31 |
| ES2183923T3 (es) | 2003-04-01 |
| CA2174707A1 (en) | 1996-10-25 |
| CA2174707C (en) | 2008-03-25 |
| KR960037680A (ko) | 1996-11-19 |
| KR100416674B1 (ko) | 2004-06-11 |
| RU2156250C2 (ru) | 2000-09-20 |
| CN1063176C (zh) | 2001-03-14 |
| AU5080596A (en) | 1996-11-07 |
| IL117989A (en) | 2000-01-31 |
| EP0739892A3 (de) | 1997-01-22 |
| DE59609707D1 (de) | 2002-10-31 |
| EP0739892B1 (de) | 2002-09-25 |
| EP0739892A2 (de) | 1996-10-30 |
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| Date | Code | Title | Description |
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| GD4A | Issue of patent certificate for granted invention patent | ||
| MM4A | Annulment or lapse of patent due to non-payment of fees |